首页> 外文期刊>The journal of clinical psychiatry >Social phobia: etiology, neurobiology, and treatment.
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Social phobia: etiology, neurobiology, and treatment.

机译:社交恐惧症:病因,神经生物学和治疗。

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Social phobia is a common and often disabling condition, with an etiology that is not established. There is evidence at several levels for an interplay of biological and psychological processes in social phobia. Genetic studies show that both genetic and environmental factors are important, with evidence pointing to associations with 2 genetic conditions, autism and fragile X syndrome. Behavioral inhibition has emerged as an important precursor to social phobia and possibly to other anxiety disorders. Epidemiologic and clinical studies have suggested that factors within the family environment, such as overprotection, overcontrol, modeling of anxiety, criticism, and in some cases abuse, can play a role in the development of social phobia. During childhood, complex interactions between brain system disturbances that mediate responses to negative social cues and factors in the social setting may lead to the development of a distorted set of internal "blueprints" for social behavior. The impact of severe social anxiety on brain systems that mediate behavioral change may prevent patients from learning better blueprints. The effective control of social anxiety with medications enables patients to recover; whether recovery can last after discontinuation of medications may depend on whether a new "blueprint" has been developed and whether stable changes in affected brain systems have occurred. Neuroimaging techniques are at the early stage of identifying abnormalities at the neurotransmitter and systems levels.
机译:社交恐惧症是一种常见且常常致残的疾病,其病因尚不明确。在几个层面上,都有证据表明社交恐惧症中的生物学和心理过程相互影响。遗传研究表明,遗传因素和环境因素都很重要,证据表明与自闭症和脆弱X综合征这2种遗传状况相关。行为抑制已成为社交恐惧症和其他焦虑症的重要先兆。流行病学和临床研究表明,家庭环境中的因素,例如过度保护,过度控制,焦虑模型,批评以及在某些情况下的虐待,可能在社交恐惧症的发展中起作用。在儿童时期,介导对负面社交线索和社交环境因素的响应的大脑系统干扰之间的复杂相互作用可能会导致一组扭曲的内部“蓝图”用于社交行为的发展。严重的社交焦虑对介导行为改变的大脑系统的影响可能会阻止患者学习更好的蓝图。用药物有效控制社交焦虑症可使患者康复;停药后恢复是否能持续取决于新的“蓝图”是否已开发以及受影响的脑系统是否发生了稳定的变化。神经成像技术处于识别神经递质和系统水平异常的早期阶段。

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